Core-Binding Factor Influences the Disease Specificity of Moloney Murine Leukemia Virus

The core site in the Moloney murine leukemia virus (Moloney MLV) enhancer was previously shown to be an important determinant of the T-cell disease specificity of the virus. Mutation of the core site resulted in a significant shift in disease specificity of the Moloney virus from T-cell leukemia to erythroleukemia. We and others have since determined that a protein that binds the core site, one of the core-binding factors (CBF) is highly expressed in thymus and is essential for hematopoiesis. Here we test the hypothesis that CBF plays a critical role in mediating pathogenesis of Moloney MLV in vivo. We measured the affinity of CBF for most core sites found in MLV enhancers, introduced sites with different affinities for CBF into the Moloney MLV genome, and determined the effects of these sites on viral pathogenesis. We found a correlation between CBF affinity and the latent period of disease onset, in that Moloney MLVs with high-affinity CBF binding sites induced leukemia following a shorter latent period than viruses with lower-affinity sites. The T-cell disease specificity of Moloney MLV also appeared to correlate with the affinity of CBF for its binding site. The data support a role for CBF in determining the pathogenic properties of Moloney MLV.     

Nitrogen and carbon isotope fractionation between mothers, neonates, and nursing offspring

Stable isotope signatures of lactating females and their nursing offspring were measured on 11 species, including herbivores, carnivores, hibernators, and non-hibernators. We hypothesized that: (1) nursing offspring would have stable isotope signatures that were a trophic level higher than their mothers, and (2) this pattern would be species-independent. The plasma of adult females had a '¹⁵N enrichment over their diets of 4.1ǂ.7‰, but offspring plasma had a mean '¹⁵N enrichment over maternal plasma of 0.9ǂ.8‰ and no C enrichment (0.0ǂ.6‰). The trophic level enrichment did not occur between mother and offspring because milk was depleted in both '¹⁵N (1.0ǂ.5‰) and '¹³C (2.1ǂ.9‰) relative to maternal plasma. Milk to offspring plasma enrichment was relatively small ('¹⁵N enrichment of 1.9ǂ.7‰ and '¹³C enrichment of 1.9ǂ.8‰) compared to the trophic level enrichment between the adults and their diets. While some species did have significant differences between the isotope signatures of mother and offspring, the differences were not related to whether they were hibernators or non-hibernators, carnivores or herbivores. Investigators wanting to use stable isotopes to quantify weaning or other lactation processes or diets of predators when both adults and nursing offspring are consumed must first establish the parameters that apply to a particular species/environment/diet combination.